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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
1

The eicosanoid response to high dose UVR exposure of individuals prone and resistant to sunburn

Nicolaou, Anna, Masoodi, Mojgan, Gledhill, Karl, Haylett, A.K., Thody, Anthony J., Tobin, Desmond J., Rhodes, L.E. January 2012 (has links)
No / High personal UVR doses can be gained during leisure activities, causing intense self-resolving inflammation (sunburn) of unprotected skin. UVR activates release of membrane fatty acids and upregulates their metabolism by cyclooxygenases (COX) and lipoxygenases (LOX) to different eicosanoids. While COX-derived prostaglandin (PG)E2 is a potent mediator of sunburn vasodilatation, LOX-derived 15-hydroxyeicosatetraenoic acid (HETE) and its lipoxin metabolites may contribute to sunburn limitation. We explored the relationships between expression of these lipid mediators and the clinical and histological outcomes, comparing responses of individuals prone and more resistant to sunburn. An acute UVR exposure of 12 SED (standard erythema dose) was applied to buttock skin of 32 white Caucasians (n = 16 phototype I/II, n = 16 phototype III/IV), and over the subsequent 72 h assessments were made of skin erythema, immunohistochemical expression of leukocyte markers, COX-2, 12-LOX, 15-LOX and nitric oxide synthase (NOS), and eicosanoid levels by LC/ESI-MS/MS. Evidence of a significant inflammatory response was seen earlier in phototype I/II with regard to expression of erythema (4h, p < 0.001), neutrophil infiltration (24 h, p = 0.01), epidermal COX-2 (24 h, p < 0.05) and 12-LOX (24 h, p < 0.01), and dermal eNOS (24 h, p < 0.05) proteins, although CD3+ lymphocyte infiltration showed an earlier increase in phototype III/IV (24 h, p < 0.05). Although erythema was equivalent at 72 h in both groups, phototype I/II showed higher PGE2 accompanied by elevated 15-HETE, and a strong positive correlation was seen between these mediators (n = 18, r = 0.805, p = 0.0001). Hence anti-inflammatory eicosanoid 15-HETE may temper the pro-inflammatory milieu in sunburn, having greater influence in those prone to sunburn than those more resistant, given the same high UVR exposure conditions. / The Wellcome Trust
2

Rôles et régulations des canaux ioniques ASIC3 dans la douleur / Roles and regulation of ion channel ASIC3 in pain

Delaunay, Anne 30 October 2013 (has links)
Les douleurs chroniques, d’origine inflammatoire, neuropathique ou incisionnelle, affectent environ 20 % de la population adulte et jusqu’à 50 % de la population âgée. Elles représentent ainsi un véritable enjeu de santé publique. Malgré l’existence de grandes familles d’analgésiques, les traitements restent souvent inefficaces. Cela est dû en grande partie à un manque de connaissances des mécanismes physiopathologiques de la douleur. Durant ma thèse, je me suis intéressée aux rôles et aux régulations de senseurs moléculaires de la douleur récemment mis en évidence: les canaux ioniques ASIC (« Acid Sensing Ion Channels »). Les ASIC forment une famille de canaux cationiques, excitateurs. Les canaux ASIC3, en particulier, sont présents dans les neurones sensoriels qui innervent la peau, les muscles, les viscères et les articulations. Ils sont activés par de faibles acidifications extracellulaires qui se produisent au cours de nombreux mécanismes physiopathologiques comme l’inflammation, l’ischémie, le développement tumoral, ou encore les lésions tissulaires consécutives, par exemple, à une chirurgie. Dans une première étude, nous avons montré que les canaux ASIC3 jouent un rôle primordial dans le développement des douleurs post-opératoires, notamment dans les douleurs posturales, proches des cas cliniques. A partir d’un modèle d’incision plantaire chez le rat, nous avons mis en évidence une surexpression des canaux ASIC3 dans les neurones sensoriels qui innervent la patte opérée. L’inhibition pharmacologique (toxine) et génique (siARN) d’ASIC3 in vivo réduit le comportement douloureux. Notre seconde étude a porté sur le canal ASIC3 humain, peu étudié jusqu’ici. J’ai démontré que ce canal possède une propriété originale et inductible qui lui confère une sensibilité, non seulement à l’acidification, mais également à l’alcalinisation extracellulaire. Cette sensibilité alcaline est une caractéristique intrinsèque du canal. Elle implique deux résidus arginine spécifiques à la protéine humaine et présents sur sa boucle extracellulaire. Le canal ASIC3 humain, en adaptant son activité à différents environnements de pH, pourrait ainsi participer à la régulation fine du potentiel de membrane et à la sensibilisation neuronale. Plus récemment, j’ai étudié la régulation du canal ASIC3 par des lipides inflammatoires et ses conséquences sur la douleur. De manière très intéressante, je démontre que la lysophosphatidylcholine (LPC), un lipide issu de la dégradation membranaire lors de processus inflammatoires, est un nouvel activateur du canal ASIC3 en conditions normales de pH. De plus, en synergie avec une acidose modérée (pH 7,0), la LPC et son analogue non métabolisable produisent une douleur spontanée chez les rats, qui est réduite en présence de toxine inhibitrice d’ASIC3. / Chronic, inflammatory, neuropathic, or incisional pain is affecting about 20 % of the adult population and up to 50 % of the elderly population. It thus represent a real public health issue. Despite the existence of large families of analgesics, treatments are often ineffective. This is due in large part to a lack of knowledge of the patho-physiological mechanisms of pain. During my PhD, I have been interested in the roles and regulation of molecular sensors of the pain recently highlighted: ion channels (ASICs "Acid Sensing Ion Channels "). ASICs constitute a family of excitatory cationic channels. The ASIC3 channels, in particular, are present in sensory neurons that innervate the skin, muscles, organs and joints. They are activated by low extracellular acidification occurring in many patho-physiological mechanisms such as inflammation, ischemia, tumor growth, or the subsequent tissue damage, for example, surgery. In a first study, we showed that ASIC3 channels play a crucial role in the development of post -operative pain, including postural pain, close to clinical cases. From a plantar incision model in rats, we demonstrated an over-expression of ASIC3 channels in sensory neurons innervating the operated hindpaw. Pharmacological inhibition (with toxin) and invalidation (siRNA) of ASIC3 in vivo reduce pain behavior. Our second study focused on the human ASIC3 channel, not yet extensively studied. I demonstrated that this channel has a unique and inducible property which gives it a sensitivity not only to acidification, but also to the extracellular alkalinization. This alkaline sensitivity is an intrinsic characteristic of the channel. It involves two specific arginine residues in the human channel that are present in its extracellular loop.Thus the human ASIC3 channel adapts its activity at different pH environments, and could participate in the fine regulation of membrane potential and neuronal sensitization. More recently, I have studied the regulation of ASIC3 channel by inflammatory lipids and there effects on pain. Interestingly, I showed that lysophosphatidylcholine (LPC), a lipid produced from the degradation of the membrane during inflammation, is a new activator of ASIC3 channel under normal pH conditions. Moreover, in synergy with moderate acidosis (pH 7.0), the LPC and its non-metabolizable analogue produce spontaneous pain in rats. This pain is reduced in the presence of the ASIC3 inhibitory toxin.

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